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Mouse ENU Mutagenesis to Understand Immunity to Infection: Methods, Selected Examples, and Perspectives

Infectious diseases are responsible for over 25% of deaths globally, but many more individuals are exposed to deadly pathogens. The outcome of infection results from a set of diverse factors including pathogen virulence factors, the environment, and the genetic make-up of the host. The completion of...

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Autores principales: Caignard, Grégory, Eva, Megan M., van Bruggen, Rebekah, Eveleigh, Robert, Bourque, Guillaume, Malo, Danielle, Gros, Philippe, Vidal, Silvia M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4276919/
https://www.ncbi.nlm.nih.gov/pubmed/25268389
http://dx.doi.org/10.3390/genes5040887
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author Caignard, Grégory
Eva, Megan M.
van Bruggen, Rebekah
Eveleigh, Robert
Bourque, Guillaume
Malo, Danielle
Gros, Philippe
Vidal, Silvia M.
author_facet Caignard, Grégory
Eva, Megan M.
van Bruggen, Rebekah
Eveleigh, Robert
Bourque, Guillaume
Malo, Danielle
Gros, Philippe
Vidal, Silvia M.
author_sort Caignard, Grégory
collection PubMed
description Infectious diseases are responsible for over 25% of deaths globally, but many more individuals are exposed to deadly pathogens. The outcome of infection results from a set of diverse factors including pathogen virulence factors, the environment, and the genetic make-up of the host. The completion of the human reference genome sequence in 2004 along with technological advances have tremendously accelerated and renovated the tools to study the genetic etiology of infectious diseases in humans and its best characterized mammalian model, the mouse. Advancements in mouse genomic resources have accelerated genome-wide functional approaches, such as gene-driven and phenotype-driven mutagenesis, bringing to the fore the use of mouse models that reproduce accurately many aspects of the pathogenesis of human infectious diseases. Treatment with the mutagen N-ethyl-N-nitrosourea (ENU) has become the most popular phenotype-driven approach. Our team and others have employed mouse ENU mutagenesis to identify host genes that directly impact susceptibility to pathogens of global significance. In this review, we first describe the strategies and tools used in mouse genetics to understand immunity to infection with special emphasis on chemical mutagenesis of the mouse germ-line together with current strategies to efficiently identify functional mutations using next generation sequencing. Then, we highlight illustrative examples of genes, proteins, and cellular signatures that have been revealed by ENU screens and have been shown to be involved in susceptibility or resistance to infectious diseases caused by parasites, bacteria, and viruses.
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spelling pubmed-42769192014-12-30 Mouse ENU Mutagenesis to Understand Immunity to Infection: Methods, Selected Examples, and Perspectives Caignard, Grégory Eva, Megan M. van Bruggen, Rebekah Eveleigh, Robert Bourque, Guillaume Malo, Danielle Gros, Philippe Vidal, Silvia M. Genes (Basel) Review Infectious diseases are responsible for over 25% of deaths globally, but many more individuals are exposed to deadly pathogens. The outcome of infection results from a set of diverse factors including pathogen virulence factors, the environment, and the genetic make-up of the host. The completion of the human reference genome sequence in 2004 along with technological advances have tremendously accelerated and renovated the tools to study the genetic etiology of infectious diseases in humans and its best characterized mammalian model, the mouse. Advancements in mouse genomic resources have accelerated genome-wide functional approaches, such as gene-driven and phenotype-driven mutagenesis, bringing to the fore the use of mouse models that reproduce accurately many aspects of the pathogenesis of human infectious diseases. Treatment with the mutagen N-ethyl-N-nitrosourea (ENU) has become the most popular phenotype-driven approach. Our team and others have employed mouse ENU mutagenesis to identify host genes that directly impact susceptibility to pathogens of global significance. In this review, we first describe the strategies and tools used in mouse genetics to understand immunity to infection with special emphasis on chemical mutagenesis of the mouse germ-line together with current strategies to efficiently identify functional mutations using next generation sequencing. Then, we highlight illustrative examples of genes, proteins, and cellular signatures that have been revealed by ENU screens and have been shown to be involved in susceptibility or resistance to infectious diseases caused by parasites, bacteria, and viruses. MDPI 2014-09-29 /pmc/articles/PMC4276919/ /pubmed/25268389 http://dx.doi.org/10.3390/genes5040887 Text en © 2014 by the authors; licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Review
Caignard, Grégory
Eva, Megan M.
van Bruggen, Rebekah
Eveleigh, Robert
Bourque, Guillaume
Malo, Danielle
Gros, Philippe
Vidal, Silvia M.
Mouse ENU Mutagenesis to Understand Immunity to Infection: Methods, Selected Examples, and Perspectives
title Mouse ENU Mutagenesis to Understand Immunity to Infection: Methods, Selected Examples, and Perspectives
title_full Mouse ENU Mutagenesis to Understand Immunity to Infection: Methods, Selected Examples, and Perspectives
title_fullStr Mouse ENU Mutagenesis to Understand Immunity to Infection: Methods, Selected Examples, and Perspectives
title_full_unstemmed Mouse ENU Mutagenesis to Understand Immunity to Infection: Methods, Selected Examples, and Perspectives
title_short Mouse ENU Mutagenesis to Understand Immunity to Infection: Methods, Selected Examples, and Perspectives
title_sort mouse enu mutagenesis to understand immunity to infection: methods, selected examples, and perspectives
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4276919/
https://www.ncbi.nlm.nih.gov/pubmed/25268389
http://dx.doi.org/10.3390/genes5040887
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